anosmia

Bosma Arhinia Microphthalmia Syndrome

Clinical Characteristics

Ocular Features:

Microphthalmia or clinical anophthalmia are usually present. Iris colobomas are frequent features. Occluded or absent nasolacrimal ducts have been reported.

Systemic Features:

Arhina with anosmia is the most striking feature but it is usually accompanied by midface hypoplasia, a highly arched (or cleft) palate, and preauricular pits. The nasal bones along with the cribriform plate, and other septal structures may be missing. Maxillary and paranasal sinuses, together with the olfactory bulbs are often absent. Intelligence is usually normal.

Choanal atresia is often present. Hypogonadotropic hypogonadism with micropenis and cryptorchidism is an important feature in males. Females may experience pubertal delay with menarche anomalies.

Genetics

Heterozygous mutations in the SMCHD1 gene (18p11) are responsible for this disorder. There is considerable clinical heterogeneity with many carriers having only minor manifestations.

Pedigree:

Autosomal dominant

Treatment

Treatment Options:

No treatment for the general disorder has been described.

References

Article Title:

De novo mutations in SMCHD1 cause Bosma arhinia microphthalmia syndrome and abrogate nasal development

Gordon CT, Xue S, Yigit G, Filali H, Chen K, Rosin N, Yoshiura KI, Oufadem M, Beck TJ, McGowan R, Magee AC, Altmuller J, Dion C, Thiele H, Gurzau AD, Nurnberg P, Meschede D, Muhlbauer W, Okamoto N, Varghese V, Irving R, Sigaudy S, Williams D, Ahmed SF, Bonnard C, Kong MK, Ratbi I, Fejjal N, Fikri M, Elalaoui SC, Reigstad H, Bole-Feysot C, Nitschke P, Ragge N, Levy N, Tuncbilek G, Teo AS, Cunningham ML, Sefiani A, Kayserili H, Murphy JM, Chatdokmaiprai C, Hillmer AM, Wattanasirichaigoon D, Lyonnet S, Magdinier F, Javed A, Blewitt ME, Amiel J, Wollnik B, Reversade B. De novo mutations in SMCHD1 cause Bosma arhinia microphthalmia syndrome and abrogate nasal development. Nat Genet. 2017 Feb;49(2):249-255.

PubMed ID:

28067911

Bosma arhinia microphthalmia syndrome: Clinical report and review of the literature

Brasseur B, Martin CM, Cayci Z, Burmeister L, Schimmenti LA. Bosma arhinia microphthalmia syndrome: Clinical report and review of the literature. Am J Med Genet A. 2016 May;170A(5):1302-7.

PubMed ID:

26842768

Kufor-Rakeb Syndrome

Clinical Characteristics

Ocular Features:

Most patients have a supranuclear gaze paresis. Patients later may have dystonic oculogyric spasms.

Systemic Features:

This is a rapidly progressive neurodegenerative disorder with juvenile onset. First signs of Parkinisonism are evident between the ages of 12 and 16 years of age. Within a year of onset severe motor handicaps develop along with some degree of dementia with aggression and visual hallucinations. Cognitive decline is often a feature. Fine tremors in the chin may be seen along with other extrapyramidal signs but these are not prominent in the limbs. Instead there is often rigidity and bradykinesia. Dysphagia, dysarthria, and ataxia are features in many patients. Peripheral sensory neuropathy and anosmia are present in some individuals.

Brain imaging often reveals generalized atrophy of the cerebellum, cerebral cortex, and brainstem.

Genetics

This condition results from homozygous or compound heterozygous mutations in the ATP13A2 gene (1p36.13).

Biallelic mutations in the same gene are also responsible for spastic paraplegia 78 (617225) with somewhat similar clinical features except for the general absence of Parkinsonism.

Pedigree:

Autosomal recessive

Treatment

Treatment Options:

There may be an initial therapeutic response to L-DOPA but this is often not maintained

References

Article Title:

Loss-of-function mutations in the ATP13A2/PARK9 gene cause complicated hereditary spastic paraplegia (SPG78)

Estrada-Cuzcano A, Martin S, Chamova T, Synofzik M, Timmann D, Holemans T, Andreeva A, Reichbauer J, De Rycke R, Chang DI, van Veen S, Samuel J, Schols L, Poppel T, Mollerup Sorensen D, Asselbergh B, Klein C, Zuchner S, Jordanova A, Vangheluwe P, Tournev I, Schule R. Loss-of-function mutations in the ATP13A2/PARK9 gene cause complicated hereditary spastic paraplegia (SPG78). Brain. 2017 Feb;140(Pt 2):287-305.

PubMed ID:

28137957

Kufor Rakeb disease: autosomal recessive, levodopa-responsive parkinsonism with pyramidal degeneration, supranuclear gaze palsy, and dementia

Williams DR, Hadeed A, al-Din AS, Wreikat AL, Lees AJ. Kufor Rakeb disease: autosomal recessive, levodopa-responsive parkinsonism with pyramidal degeneration, supranuclear gaze palsy, and dementia. Mov Disord. 2005 Oct;20(10):1264-71.

PubMed ID:

15986421

Refsum Disease, Adult

Clinical Characteristics

Ocular Features:

A retinitis pigmentosa-like retinopathy is the major ocular manifestation of this disease. There is typical night blindness and visual field constriction. Rod ERG responses are usually subnormal. However, central acuity is also reduced due to a degenerative maculopathy. Cataracts and optic atrophy are common. The macula may undergo progressive degeneration and optic atrophy is not uncommon. Some patients have defective pupillary responses.

Systemic Features:

Onset of symptoms is usually late in the first decade and sometimes into the third decade. There is usually a polyneuropathy with impaired motor reflexes and paresis in the limbs. A progressive sensorineural hearing loss occurs in many patients. Sensory deficits also occur. Some have ataxia and skin changes of ichthyosis. Anosmia is a near universal feature. Heart failure may occur and cardiac abnormalities such as conduction defects can occur. A variety of skeletal abnormalities such as pes cavus, short fourth metatarsals, and evidence of epiphyseal dysplasia have been reported. There is considerable clinical heterogeneity even within families.

Phytanic acid oxidase activity as measured in fibroblasts is often low while serum phytanic acid is increased. The cerebrospinal fluid contains increased protein but no increase in cells.

Genetics

This disorder results from mutations in the PHYH (PAHX) gene (10pter-p11.2) encoding phytanoyl-CoA hydroxylase, or, more rarely in PEX7 (6q22-q24) encoding peroxin-7 resulting in an uncommon condition (10% of cases) sometimes called adult Refsum disease-2.

Mutations in the latter gene also cause rhizomelic chondrodysplasia punctata type 1 (215100) which does not have all of the neurological features or the retinopathy.

There is also so-called infantile form of Refsum disease (266510).

Pedigree:

Autosomal recessive

Treatment

Treatment Options:

A diet low in phytanic acid can lead to improvement in the neurologic symptoms such as the ataxia and polyneuropathy but must be instituted in early stages of the disease. This approach may not be as beneficial for the visual or auditory symptoms.

References

Article Title:

Identification of PEX7 as the second gene involved in Refsum disease

van den Brink DM, Brites P, Haasjes J, Wierzbicki AS, Mitchell J, Lambert-Hamill M, de Belleroche J, Jansen GA, Waterham HR, Wanders RJ. Identification of PEX7 as the second gene involved in Refsum disease. Am J Hum Genet. 2003 Feb;72(2):471-7.

PubMed ID:

12522768

Human phytanoyl-CoA hydroxylase: resolution of the gene structure and the molecular basis of Refsum's disease

Jansen GA, Hogenhout EM, Ferdinandusse S, Waterham HR, Ofman R, Jakobs C, Skjeldal OH, Wanders RJ. Human phytanoyl-CoA hydroxylase: resolution of the gene structure and the molecular basis of Refsum's disease. Hum Mol Genet. 2000 May 1;9(8):1195-200.

PubMed ID:

10767344

Clinical and biochemical heterogeneity in conditions with phytanic acid accumulation

Skjeldal OH, Stokke O, Refsum S, Norseth J, Petit H. Clinical and biochemical heterogeneity in conditions with phytanic acid accumulation. J Neurol Sci. 1987 Jan;77(1):87-96.

PubMed ID:

2433405

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